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Featured researches published by Satoshi Takeo.


Journal of Biological Chemistry | 2010

Stable Interaction between the Human Proliferating Cell Nuclear Antigen Loader Complex Ctf18-Replication Factor C (RFC) and DNA Polymerase ϵ Is Mediated by the Cohesion-specific Subunits, Ctf18, Dcc1, and Ctf8

Takeshi Murakami; Ryuji Takano; Satoshi Takeo; Rina Taniguchi; Kaori Ogawa; Eiji Ohashi; Toshiki Tsurimoto

One of the proliferating cell nuclear antigen loader complexes, Ctf18-replication factor C (RFC), is involved in sister chromatid cohesion. To examine its relationship with factors involved in DNA replication, we performed a proteomics analysis of Ctf18-interacting proteins. We found that Ctf18 interacts with a replicative DNA polymerase, DNA polymerase ϵ (pol ϵ). Co-immunoprecipitation with recombinant Ctf18-RFC and pol ϵ demonstrated that their binding is direct and mediated by two distinct interactions, one weak and one stable. Three subunits that are specifically required for cohesion in yeast, Ctf18, Dcc1, and Ctf8, formed a trimeric complex (18-1-8) and together enabled stable binding with pol ϵ. The C-terminal 23-amino acid stretch of Ctf18 was necessary for the trimeric association of 18-1-8 and was required for the stable interaction. The weak interaction was observed with alternative loader complexes including Ctf18-RFC(5), which lacks Dcc1 and Ctf8, suggesting that the common loader structures, including the RFC small subunits (RFC2–5), are responsible for the weak interaction. The two interaction modes, mediated through distinguishable structures of Ctf18-RFC, both occurred through the N-terminal half of pol ϵ, which includes the catalytic domain. The addition of Ctf18-RFC or Ctf18-RFC(5) to the DNA synthesis reaction caused partial inhibition and stimulation, respectively. Thus, Ctf18-RFC has multiple interactions with pol ϵ that promote polymorphic modulation of DNA synthesis. We propose that their interaction alters the DNA synthesis mode to enable the replication fork to cooperate with the establishment of cohesion.


Chemical & Pharmaceutical Bulletin | 1971

Synthesis of 1, 5-Benzothiazepine Derivatives. III

Hiroshi Kugita; Hirozumi Inoue; Muneyoshi Ikezaki; Mikihiko Konda; Satoshi Takeo


Chemical & Pharmaceutical Bulletin | 1970

Synthesis of 1,5-Benzothiazepine Derivatives. I

Hiroshi Kugita; Hirozumi Inoue; Muneyoshi Ikezaki; Satoshi Takeo


Chemical & Pharmaceutical Bulletin | 1970

Synthesis of 1, 5-Benzothiazepine Derivatives. II

Hiroshi Kugita; Hirozumi Inoue; Muneyoshi Ikezaki; Mikihiko Konda; Satoshi Takeo


Chemical & Pharmaceutical Bulletin | 1977

Studies on Tertiary Amine Oxides. LXI. Some Reactions of 2-Phenylquinoline 1-Oxide and Its Derivatives

Masatomo Hamana; Satoshi Takeo; Hiroshi Noda


Archive | 1973

PROCESSO PARA A PREPARACAO DE DERIVADOS DE BENZO-TIAZEPIN

Muneyoshi Ikezaki; Satoshi Takeo; Hiroshi Kugita; Hirozumi Inoue


Archive | 1972

Verfahren zur Herstellung von neuen Bezothiazepinderivaten

Hiroshi Kugita; Satoshi Takeo; Masanori Sato; Taku Nagao


Archive | 1970

1,5-benzothiazepine derivatives and processes for their preparation

Hiroshi Kugita; Satoshi Takeo; Taku Nagao; Masanori Sato


Archive | 1970

1,5-Benzothiazepinderivate und Verfahren zu ihrer Herstellung 1,5-benzothiazepine derivatives and processes for their preparation

Hiroshi Kugita; Satoshi Takeo; Taku Nagao; Masanori Sato


Archive | 1968

Benzothiazepine derivatives, their salts and processes for their preparation

Hiroshi Kugita; Hirozumi Inoue; Muneyoshi Ikezaki; Satoshi Takeo

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Hirozumi Inoue

National Institutes of Health

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